Treatment of tauopathies
Abstract
The invention is directed to methods of treatment of Alzheimer's disease and other tauopathies, via the administration of antibodies having specificity to abnormal forms of tau protein, the antibodies showing no binding and/or reactivity to a normal tau protein and being administered under conditions and in amounts effective to prevent or treat Alzheimer's disease or other tauopathies. In certain embodiments, the antibodies are selective for soluble truncated tau protein truncated at (i) its C-terminus after the glutamic acid residue Glu391, or (ii) at the aspartic acid residue Asp421, or (iii) at its N-terminus at the aspartic acid residue Asp13, or (iv) a combination of (i)-(iii). Further aspects of the invention are directed to the administration of an immunogen comprising an abnormal tau, preferably a soluble truncated tau.
Claims
exact text as granted — not AI-modified1 - 66 . (canceled)
67 . A method of slowing the progression or ameliorating a symptom of a tauopathy in a human, comprising administering an antibody to a human in need of therapy for the tauopathy in an amount effective to delay the onset, slow the progression or ameliorate the symptom of the tauopathy, wherein
the tauopathy is Frontotemporal dementia, and the antibody binds an artificial peptide consisting of SEQ ID NOs. 78-86 with an equilibrium constant KD from 1×10 −9 M to 1×10 −11 M, as measured by the surface plasmon resonance assay utilizing peptide captured on streptavidin chip, but does not bind hTau40.
68 . The method of claim 67 , wherein the antibody is TauC3.
69 . The method of claim 68 , wherein the antibody is administered in a pharmaceutical formulation comprising (i) TauC3 and (ii) one or more pharmaceutically acceptable excipient(s).
70 . The method of claim 69 , wherein one of the pharmaceutically acceptable excipients is a diluent.
71 . The method of claim 67 , wherein the antibody has an equilibrium constant KD with hTau40 which is from 1×10 −4 M to 1×10 −6 M, as measured by the surface plasmon resonance assay utilizing peptide captured on streptavidin chip.
72 . The method of claim 67 , wherein the antibody shows no detectable binding with hTau40, as measured by immunoblot.
73 . The method of claim 67 , wherein the antibody is administered via an IV infusion.
74 . A method of inhibiting tau polymerization in vivo, comprising administering to a human in need of therapy for Frontotemporal dementia an effective amount of an antibody showing no reactivity and/or binding with a normal tau protein, and being administered in an amount effective to inhibit polymerization of tau in the brain of the human, wherein
the normal tau protein is hTau40, the antibody binds an artificial peptide consisting of a sequence identical or homologous to SEQ ID Nos. 78-86, but does not recognize hTau40, provided that if the antibody binds a sequence homologous to SEQ ID. NO. 84 or 85, the sequence homologous to SEQ ID. NO. 84 or 85 is not phosphorylated.
75 . The method of claim 74 , wherein the antibody is TauC3.
76 . The method of claim 75 , wherein the antibody is administered in a pharmaceutical formulation comprising (i) TauC3 and (ii) one or more pharmaceutically acceptable excipient(s).
77 . The method of claim 76 , wherein one of the pharmaceutically acceptable excipients is a diluent.
78 . The method of claim 74 , wherein the antibody is administered via an IV infusion.
79 . The method of claim 74 , wherein the antibody has an equilibrium constant KD with hTau40 which is from 1×10 −4 M to 1×10 −6 M, as measured by the surface plasmon resonance assay utilizing peptide captured on streptavidin chip.
80 . The method of claim 74 , wherein the antibody has an equilibrium constant KD with the sequence identical or homologous to SEQ ID Nos. 78-86 of from 1×10 −9 M to 1×10 −11 M, as measured by the surface plasmon resonance assay utilizing peptide captured on streptavidin chip.
81 . A method of slowing progression of a tangle-related behavioral phenotype in a subject, comprising administering antibodies to a human in need of therapy for Frontotemporal dementia, the antibodies having specificity to abnormal forms of tau proteins and showing no binding and/or reactivity with a normal tau protein, the antibodies being administered under conditions and in an amount(s) effective to slow a tangle-related behavioral phenotype in a subject, wherein
the abnormal forms of tau proteins comprise hTau40 truncated at the aspartic acid residue Asp421, the normal tau protein is a full length untruncated hTau40, the antibodies specifically recognize a sequence out of SEQ ID NOs. 78-86 in the abnormal forms of tau proteins, but do not recognize the same sequence of amino acids when present internally in the normal tau protein.
82 . The method of claim 81 , wherein the antibodies comprise TauC3.
83 . The method of claim 82 , wherein the antibodies are administered in a pharmaceutical formulation comprising (i) TauC3 and (ii) one or more pharmaceutically acceptable excipient(s).
84 . The method of claim 83 , wherein one of the pharmaceutically acceptable excipients is a diluent.
85 . The method of claim 81 , wherein the antibodies are administered via an IV infusion.
86 . The method of claim 67 , further comprising accessing efficacy of the antibody by PET or MRI.Join the waitlist — get patent alerts
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